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首页> 外文期刊>Central European Journal of Chemistry >Synthesis and characterization of molecularly imprinted polymer for controlled release of tramadol
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Synthesis and characterization of molecularly imprinted polymer for controlled release of tramadol

机译:曲马多控释分子印迹聚合物的合成与表征

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摘要

In this paper, we describe how to prepare a highly selective imprinted polymer by a bulk polymerization technique. We used tramadol as the template, (MAA) as functional monomers, and (EGDMA) as the cross-linker in chloroform as solvent. Results from Fourier Transform Infrared Spectroscopy (FTIR), Thermogravimetric Analysis (TGA), Scanning Electron microscopy (SEM) show that this imprinted sorbent exhibits good recognition and high affinity for tramadol. Selectivity of molecularly imprinted polympers (MIP) was evaluated by comparing several substances with similar molecular structures to that of tramadol. Controlled release of tramadol from MIPs was investigated through in vitro dissolution tests and by measuring the absorbance at λ_(max) of 272 nm by (HPLC-UV). The dissolution media employed were hydrochloric acid pH 3.0 and phosphate buffers, pH 5.0 and 7.4, maintained at 37 and 25 ± 0.5℃. The results show the ability of MIP polymers to control tramadol release. In all cases, the release of MIPs was deferred for a longer time as compared to NMIP. At a pH of 7.4 and 25℃ slower release of tramadol imprinted polymer occurred.
机译:在本文中,我们描述了如何通过本体聚合技术制备高选择性印迹聚合物。我们使用曲马多作为模板,(MAA)作为功能性单体,(EGDMA)作为氯仿中的交联剂作为溶剂。傅里叶变换红外光谱(FTIR),热重分析(TGA),扫描电子显微镜(SEM)的结果表明,这种印迹吸附剂对曲马多具有良好的识别性和高亲和力。通过比较几种分子结构与曲马多相似的物质,可以评估分子印迹多聚物(MIP)的选择性。通过体外溶出度测试和通过(HPLC-UV)测量272 nm的λ_(max)在吸光度下研究了曲马多从MIP的控制释放。使用的溶解介质为盐酸pH 3.0和磷酸盐缓冲液pH 5.0和7.4,维持在37和25±0.5℃。结果显示了MIP聚合物控制曲马多释放的能力。在所有情况下,与NMIP相比,MIP的发布被推迟了更长的时间。在7.4和25℃的pH值下,曲马多印迹聚合物的释放较慢。

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